Magnetic resonance imaging apparatus and magnetic resonance imaging method

ABSTRACT

A magnetic resonance imaging apparatus includes a spectrum acquisition unit and a determining unit. The spectrum acquisition unit acquires a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object. The determining unit determines one of the numbers of integrations and phase encodes of magnetic resonance signals for obtaining the frequency spectrum depending on a factor influencing the frequency spectrum.

BACKGROUND OF THE INVENTION

1. Field of the Invention

The present invention relates to a MRI (magnetic resonance imaging) apparatus and a magnetic resonance imaging method which excite nuclear spin of an object magnetically with a RF (radio frequency) signal having the Larmor frequency and reconstruct an image based on NMR (nuclear magnetic resonance) signals generated due to the excitation, and more particularly, to a magnetic resonance imaging apparatus and a magnetic resonance imaging method which make it possible to acquire a frequency spectrum of magnetic resonance signals from a metabolic product in the object by MRS (Magnetic Resonance Spectroscopy).

2. Description of the Related Art

Magnetic Resonance Imaging is an imaging method which excites nuclear spin of an object set in a static magnetic field with a RF signal having the Larmor frequency magnetically and reconstruct an image based on NMR signals generated due to the excitation.

In recent years, ¹H-MRS is performed as efficient means for early diagnosis of disease (especially, determination of the extent of a tumor). ¹H-MRS uses a magnetic resonance phenomenon to observe a frequency spectrum of magnetic resonance signals from a minute metabolite containing ¹H nuclei in a living body, and can observe NAA (N-acetylaspartate), Cho (choline), PCr/Cr (creatine phosphate/creatine), Glx (glutamic acid and glutamine), Lac (lactic acid), ml (myoinositol) and the like. The concentration of a proton metabolite such as NAA in a living body is small by about quadruple digits compared to that of biological water and metabolites distribute within 5 ppm. Therefore, it is important, in the ¹H-MRS, to properly set the voxel size to be a MRS target and the number-of-times-of-integration of echo signals for generating a spectrum so as to acquire a spectrum having narrow line widths with an improved S/N (signal to noise) ratio. The same applies to another MRS such as ³¹P-MRS and ¹³C-MRS.

Note that, as the related art of MRS, a technique has been known that alternatively performs plural pulse sequences for acquiring magnetic resonance data with regard to the concentrations of labeled glucose, unlabeled glucose, labeled compound and unlabeled compound (see, for example, Japanese Patent Application (Laid-Open disclosure) No. 2000-14657). According to this technique, the metabolic rates of glucose and its compound can be measured without blood sampling very burdensome for the object.

However, the voxel size and the number-of-times-of-integration had been conventionally set depending on experience of an operator though it is important to properly set the voxel size and the number-of-times-of-integration in MRS as described above. Accordingly, it is difficult to properly set the voxel size and the number-of-times-of-integration when the sensitivity of the RF coil or the susceptibility of the object is not uniform. As a result, an actual examination may result in failure due to a body motion or an examination time may increase unnecessarily. Accordingly, there is an issue of unnecessarily increasing an examination time.

These problems can not be solved even by the above-described conventional technology.

SUMMARY OF THE INVENTION

The present invention has been made in light of the conventional situations, and it is an object of the present invention to provide a magnetic resonance imaging apparatus and a magnetic resonance imaging method which make it possible to save useless examination time by MRS satisfactorily.

The present invention provides a magnetic resonance imaging apparatus comprising: a spectrum acquisition unit configured to acquire a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and a determining unit configured to determine one of the number of times of integrations and the number of times of phase encodes of magnetic resonance signals for obtaining the frequency spectrum depending on a factor influencing the frequency spectrum, in an aspect to achieve the object.

The present invention also provides a magnetic resonance imaging apparatus comprising: a spectrum acquisition unit configured to acquire a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and an acquisition condition changing unit configured to change an acquisition condition of the frequency spectrum during acquiring the frequency spectrum, in an aspect to achieve the object.

The present invention also provides a magnetic resonance imaging method comprising: acquiring a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and determining one of the number of times of integrations and the number of times of phase encodes of magnetic resonance signals for obtaining the frequency spectrum depending on a factor influencing the frequency spectrum, in an aspect to achieve the object.

The present invention also provides a magnetic resonance imaging method comprising: acquiring a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and changing an acquisition condition of the frequency spectrum during acquiring the frequency spectrum, in an aspect to achieve the object.

The magnetic resonance imaging apparatus and the magnetic resonance imaging method according to the present invention as described above make it possible to save useless examination time by MRS satisfactorily.

BRIEF DESCRIPTION OF THE DRAWINGS

In the accompanying drawings:

FIG. 1 is a block diagram showing a magnetic resonance imaging apparatus according to a first embodiment of the present invention;

FIG. 2 is a diagram showing an example of detail structure of the RF coil shown in FIG. 1;

FIG. 3 is a diagram showing an example arrangement of the surface coils set on the body surface side of the object shown in FIG. 2;

FIG. 4 is a diagram showing an example arrangement of the surface coils set on the back surface side of the object shown in FIG. 2;

FIG. 5 is a diagram showing another example arrangement of the surface coils set on the body surface side of the object shown in FIG. 2;

FIG. 6 is a diagram showing another example arrangement of the surface coils set on the back surface side of the object shown in FIG. 2;

FIG. 7 is a functional block diagram of the computer shown in FIG. 1;

FIG. 8 is a flowchart explaining processing for generating a RF coil sensitivity distribution by the RF coil sensitivity distribution generating unit shown in FIG. 7;

FIG. 9 is a diagram showing a RF coil sensitivity distribution generated by the RF coil sensitivity distribution generating unit shown in FIG. 7;

FIG. 10 is a flowchart explaining processing for calculating the number of times of integrations by the number-of-times-of-integration generating unit shown in FIG. 7;

FIG. 11 is a diagram showing an example of displayed arbitrary image used for a plan on MRS;

FIG. 12 is a diagram explaining a method for calculating the appropriate number of times of integrations corresponding to a size of a desired MRS target region;

FIG. 13 is a functional block diagram of computer included in a magnetic resonance imaging apparatus according to a second embodiment of the present invention;

FIG. 14 is a flowchart explaining processing for generating a uniformity distribution of a magnetic field in the magnetic resonance imaging apparatus shown in FIG. 13;

FIG. 15 is a diagram showing a magnetic field uniformity distribution generated by the magnetic field uniformity distribution generating unit shown in FIG. 13;

FIG. 16 is a flowchart explaining processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit shown in FIG. 13;

FIG. 17 is a diagram explaining a method for calculating the appropriate number of times of integrations corresponding to a size of a desired MRS target region;

FIG. 18 shows an example of configuration of a touch panel displayed for acquisition by MRS;

FIG. 19 is a functional block diagram of computer included in a magnetic resonance imaging apparatus according to a third embodiment of the present invention;

FIG. 20 is a flowchart explaining processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit shown in FIG. 19;

FIG. 21 is a diagram showing a specified region, which includes a MRS target region, for acquiring correction signals;

FIG. 22 is a diagram showing a phase shift of correction signal;

FIG. 23 is a diagram showing a shift in center frequency of correction signal with time; and

FIG. 24 is a flowchart explaining another processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit shown in FIG. 19.

DESCRIPTION OF THE PREFERRED EMBODIMENTS

A magnetic resonance imaging apparatus and a magnetic resonance imaging method according to embodiments of the present invention will be described with reference to the accompanying drawings.

1. FIRST EMBODIMENT Configuration and Function

FIG. 1 is a block diagram showing a magnetic resonance imaging apparatus according to a first embodiment of the present invention.

A magnetic resonance imaging apparatus 20 includes a static field magnet 21 for generating a static magnetic field, a shim coil 22 arranged inside the static field magnet 21 which is cylinder-shaped, a gradient coil 23 and RF coils 24.

The magnetic resonance imaging apparatus 20 also includes a control system 25. The control system 25 includes a static magnetic field power supply 26, a gradient power supply 27, a shim coil power supply 28, a transmitter 29, a receiver 30, a sequence controller 31 and a computer 32. The gradient power supply 27 of the control system 25 includes an X-axis gradient power supply 27 x, a Y-axis gradient power supply 27 y and a 2-axis gradient power supply 27 z. The computer 32 includes an input device 33, a display unit 34, a operation unit 35 and a storage unit 36.

The static field magnet 21 communicates with the static magnetic field power supply 26. The static magnetic field power supply 26 supplies electric current to the static field magnet 21 to get the function to generate a static magnetic field in a imaging region. The static field magnet 21 includes a superconductivity coil in many cases. The static field magnet 21 gets current from the static magnetic field power supply 26 which communicates with the static field magnet 21 at excitation. However, once excitation has been made, the static field magnet 21 is usually isolated from the static magnetic field power supply 26. The static field magnet 21 may Include a permanent magnet which makes the static magnetic field power supply 26 unnecessary.

The static field magnet 21 has the cylinder-shaped shim coil 22 coaxially inside itself. The shim coil 22 communicates with the shim coil power supply 28. The shim coil power supply 28 supplies current to the shim coil 22 so that the static magnetic field becomes uniform.

The gradient coil 23 includes an X-axis gradient coil 23 x, a Y-axis gradient coil 23 y and a Z-axis gradient coil 23 z. Each of the X-axis gradient coil 23 x, the Y-axis gradient coil 23 y and the Z-axis gradient coil 23 z which is cylinder-shaped is arranged inside the static field magnet 21. The gradient coil 23 has also a bed 37 in the area formed inside it which is an imaging area. The bed 37 supports an object P. The RF coils 24 include a whole body coil (WBC: whole body coil), which is built in the gantry, for transmission and reception of RF signals and local coils, which are arranged around the bed 37 or the object P, for reception of RF signals.

The gradient coil 23 communicates with the gradient power supply 27. The X-axis gradient coil 23 x, the Y-axis gradient coil 23 y and the Z-axis gradient coil 23 z of the gradient coil 23 communicate with the X-axis gradient power supply 27 x, the Y-axis gradient power supply 27 y and the Z-axis gradient power supply 27 z of the gradient power supply 27 respectively.

The X-axis gradient power supply 27 x, the Y-axis gradient power supply 27 y and the Z-axis gradient power supply 27 z supply currents to the X-axis gradient coil 23 x, the Y-axis gradient coil 23 y and the Z-axis gradient coil 23 z respectively so as to generate gradient magnetic fields Gx, Gy and Gz in the X, Y and Z directions in the imaging area.

The RF coils 24 communicate with the transmitter 29 and/or the receiver 30. The transmission RF coil 24 has a function to transmit a RF signal given from the transmitter 29 to the object P. The reception RF coil 24 has a function to receive a MR signal generated due to an nuclear spin inside the object P which is excited by the RF signal to give to the receiver 30.

FIG. 2 is a diagram showing an example of detail structures of the RF coils 24 shown in FIG. 1. FIG. 3 is a diagram showing an example arrangement of the surface coils 24 c set on the body surface side of the object P shown in FIG. 2. FIG. 4 is a diagram showing an example arrangement of the surface coils 24 c set on the back surface side of the object P shown in FIG. 2.

As shown in FIG. 2, the RF coils 24 include a cylindrical WB (whole-body) coil 24 a, and a phased array coil 24 b. The phased array coil 24 b includes a plurality of surface coils 24 c, and a plurality of the surface coils 24 c is arranged on each of the body surface side and the back surface side of the object P.

For example, as shown in FIG. 3, on the body surface side of the object P, four rows of surface coils 24 c are provided in the x-direction and eight columns of them in the z-direction, that is, a total of thirty two surface coils 24 c are arranged so as to cover a wide-ranging imaging area. Likewise, as shown in FIG. 4, on the back surface side of the object, four rows of surface coils 24 c are provided in the x-direction and eight columns of them in the z-direction, that is, a total of thirty two surface coils 24 c are arranged so as to cover a wide-ranging imaging area. On the back surface side, surface coils 24 with a smaller size than that of the other surface coils 24 c are arranged in the vicinity of the body axis from the viewpoint of sensitivity improvement, considering for the presence of the backbone of the object P.

On the other hand, the receiver 30 includes a duplexer 30 a, amplifiers 30 b, a switch composition unit 30 c, and reception circuits 30 d. The duplexer 30 a is connected to the transmitter 29, the WB coil 24 a, and the amplifier 30 b for the WB coil 24 a. The amplifiers 30 b are provided by the total number of the surface coils 24 c and the WB coil 24 a, and each connected to a respective one of the surface coils 24 c and the WB coil 24 a. The switch composition unit 30 c consists of a single piece or a plurality of pieces. The input side of the switch composition unit 30 c is connected to the plurality of surface coil units 24 c or the WB coil 24 a through the plurality of amplifiers 30 b. The reception circuits 30 d are provided by a desired number such as to be smaller than or equal to the total number of the surface coils 24 c and the WB coil 24 a, and disposed on the output side of the switch composition unit 30 c.

The WB coil 24 a can be used as a coil for the transmission of radio frequency signals. As a coil for the reception of NMR signals, each of the surface coils 24 c can be used. Furthermore, the WB coil 24 a can also be used for a receiving coil.

Therefore, the duplexer 30 a is configured so as to provide the WB coil 24 a with radio frequency signals for transmission, outputted from the transmitter 29, while providing the switch composition unit 30 c with NMR signals received in the WB coil 24 a via the amplifiers 30 b in the receiver 30. An NMR signal received in each of the surface coils 24 c is outputted to the switch composition unit 30 c via a respective one of the amplifiers 30 b.

The switch composition unit 30 c is configured so as to perform composition processing and switching with respect to NMR signals received from the surface coils 24 c or the WB coil 24 a and to output them to the corresponding reception circuits 30 d. In other words, the switch composition unit 30 c is configured so that, in conformance with the number of the reception circuits 30 d, the composition processing and switching with respect to NMR signals received from the surface coils 24 c or the WB coil 24 a are performed in the switch composition unit 30 c, and that NMR signals can be received from various imaging areas by forming sensibility distributions in response to the imaging areas, using a plurality of desired surface coils 24 c.

However, NMR signals may be received by WB coil 24 a alone without providing the surface coils 24 c. Also, NMR signals received in the surface coils 24 c or the WB coil 24 a may be directly outputted to the reception circuits 30 d without providing the switch composition unit 30 c. Furthermore, more surface coils 24 c may be extensively arranged.

FIG. 5 is a diagram showing another example arrangement of the surface coils 24 c set on the body surface side of the object P shown in FIG. 2. FIG. 6 is a diagram showing another example arrangement of the surface coils 24 c set on the back surface side of the object P shown in FIG. 2.

As shown in FIGS. 5 and 6, further more surface coils 24 c may be arranged around the object P. In an example shown in FIG. 5, three coil units 24 d each composed of sixteen elements constituted of four columns of surface coils 24 c in the x-direction and four rows of surface coils 24 c in the z-direction are arranged in the z-direction, that is, a total of forty eight elements of surface coils 24 c are arranged on the body surface side of the object P. On the other hand, in an example shown in FIG. 6, a coil unit 24 e composed of thirty two elements constituted of four columns of surface coils 24 c in the x-direction and eight rows of surface coils 24 c in the z-direction are arranged on the backbone side. of the object P; a coil units 24 f having surface coils 24 c composed of two elements (not shown) are arranged in the vicinity of jaws; and further a coil unit 24 g having surface coils 24 c composed of twelve elements (not shown) are arranged under the head, that is, a total of forty six elements of surface coils 24 c are arranged on the back surface side of the object P. Arranging the surface coils 24 c on the body surface side and back surface side of the object P as shown in FIGS. 5 and 6 results in that a total of ninety four elements of surface coils 24 c are arranged around the object P. Each of the surface coils 24 c is connected to a respective exclusive one of the amplifiers 30 b via a coil port (not shown).

Arranging a multitude of surface coils 24 c around the object P makes it possible to form a phased array coil 24 b for the whole-body, capable of receiving data from a plurality of imaging areas without moving the positions of the coils or that of the object P. Although the WB coil 24 a can also receive data from a plurality of imaging areas without moving the positions of the coils or that of the object P, the use of the phased array coil 24 b as a receiving coil allows data to be received with sensitivities more suitable for the imaging areas and with a better signal-to-noise ratio (SNR).

The sequence controller 31 of the control system 25 communicates with the gradient power supply 27, the transmitter 29 and the receiver 30. The sequence controller 31 has a function to storage sequence information describing control information needed in order to make the gradient power supply 27, the transmitter 29 and the receiver 30 drive and generate gradient magnetic fields Gx, Gy and Gz in the X, Y and Z directions and a RF signal by driving the gradient power supply 27, the transmitter 29 and the receiver 30 according to a predetermined sequence stored. The control information above-described includes motion control information, such as intensity, impression period and impression timing of the pulse electric current which should be impressed to the gradient power supply 27

The sequence controller 31 is also configured to give raw data to the computer 32. The raw data is complex data obtained through the detection of a NMR signal and A/D conversion to the NMR signal detected in the receiver 30.

The transmitter 29 has a function to give a RF signal to the RF coil 24 in accordance with control information provided from the sequence controller 31. The receiver 30 has a function to generate raw data which is digitized complex number data by detecting a MR signal given from the RF coil 24 and performing predetermined signal processing and A/P converting to the MR signal detected. The receiver 30 also has a function to give the generated raw data to the sequence controller 31.

The computer 32 gets various functions by the operation unit 35 executing some programs stored in the storage unit 36 of the computer 32. Alternatively, some specific circuits having various functions may be provided with the magnetic resonance imaging apparatus 20 instead of using some of the programs.

In addition, an ECG unit 38 for acquiring an ECG signal of the object P is provided with the magnetic resonance imaging apparatus 20. The ECG signal detected by the ECG unit 38 is outputted to the computer 32 through the sequence controller 31.

Furthermore, the bed 37 is provided with a table drive unit 39. The table drive unit 39 is connected with the computer 32 so as to move the table of the bed 37 under the control by the computer 32 for imaging with moving table method or stepping table method. The moving table method is a technique for obtaining a large FOV (field of view) in a moving direction by continuously moving the table of the bed 37 during imaging. The stepping table method is a technique for three-dimensional imaging at every station by stepping the table of the bed 37. These techniques are used in case of imaging a large area which is unable to be imaged at a time such as whole body imaging. The images acquired with moving the bed 37 may be combined mutually by compound processing in the computer 32.

FIG. 7 is a functional block diagram of the computer 32 shown in FIG. 1.

The computer 32 functions as a sequence controller control unit 41, a RF coil sensitivity distribution generating unit 42, a number-of-times-of-integration calculating unit 43 and a display data generating unit 44.

The sequence controller control unit 41 controls drive of the sequence controller 31 overall based on various information inputted by the operation of the input device 33 by an operator. The sequence controller control unit 41 provides a sequence for EPI (Echo Planar Imaging), PI (Parallel Imaging) that is imaging using the phased array coil 24 b, imaging under a gradient echo method or the like to the sequence controller 31 so that to the sequence controller 31 performs a dynamic scan.

PI is an imaging method for reducing the number of the phase encodes necessary for image reconstruction by receiving echo data with plural surface coils 24 c and skipping phase encodes. When PI is performed, information including the number of surface coils 24 c for acquiring echo data and information associating each surface coil 24 c with an imaging part necessary for PI is set as an imaging condition.

In addition, the sequence controller control unit 41 provides a sequence for ¹H-MRS in a desired MRS target region (MRS acquisition region) to the sequence controller 31 so that the sequence controller 31 performs a MRS. Of course, the sequence controller control unit 41 can make the sequence controller 31 perform a sequence for ³¹P-MRS or ¹³C-MRS.

The RF coil sensitivity distribution generating unit 42 acquires raw data provided through the sequence controller control unit 41 from the sequence controller 31 and arranges the acquired raw data in K-space (Fourier space), and also generates a RF coil sensitivity map with regard to a RF coil 24 by performing predetermined signal processing of the arranged raw data. Then, the RF coil sensitivity distribution generating unit 42 generates a RF coil sensitivity distribution indicating a change in signal intensity in an encode direction based on each signal intensity on the generated RF coil sensitivity map, and provides data including the generated RF coil sensitivity distribution to the storage unit 36.

Note that, in case of performing a MRS by PI, a RF coil sensitivity distribution is generated for each surface coil 24 c and data including RF coil sensitivity distributions corresponding to surface coils 24 c is stored in the storage unit 36.

The number-of-times-of-integration calculation unit 43 retrieves data including the RF coil sensitivity distribution stored in the storage unit 36, calculates the appropriate number-of-times-of-integration, of echo signals for generating a spectrum, corresponding to a size of a desired MRS target region by a pre-determined calculation method based on the retrieved data including the RF coil sensitivity distribution before MRS imaging, and provides data including the calculated number-of-times-of-integration to the sequence controller control unit 41.

The display data generating unit 44 displays images acquired by scans with various sequences on the display unit 34 according to a control of the sequence controller control unit 41. Specifically, the display data generating unit 44 generates display data such an image data used for a MRS plan and a frequency spectrum acquired by a MRS and displays the generated display data on the display unit 34.

Therefore, the display data generating unit 44 has a function to acquire raw data from the sequence controller control unit 41 and arrange the raw data in k-space, and a function to reconstruct image data by image reconstruction processing including FT (Fourier transformation) of k-space data arranged in k-space. Further, the display data generating unit 44 has a function to acquire echo signals acquired according to a sequence for MRS and information indicating the number-of-times-of-integration from the sequence controller control unit 41, and generate a frequency spectrum by integrating the echo signals the number of times equal to the number-of-times-of-integration.

Operation and Action

FIG. 8 is a flowchart explaining processing for generating a RF coil sensitivity distribution by the RF coil sensitivity distribution generating unit 42 shown in FIG. 7.

Next, processing for generating a RF coil sensitivity distribution by the magnetic resonance imaging apparatus 20 in FIG. 7 will be described with reference to the flowchart in FIG. 8. Note that, the processing for generating the RF coil sensitivity distribution is performed in advance as a preprocessing of processing for calculating the number-of-times-of-integration according to the present invention to be described below.

In the step S1, the sequence controller control unit 41 controls the sequence controller 31 to make the sequence controller 31 acquire data with a low resolution (for example, data with 64 times of encodes by a gradient echo method) by a gradient echo method for sensitivity correction of the RF coil 24 before MRS imaging.

The sequence controller control unit 41 provides the raw data with the low resolution acquired by the gradient echo method to the RF coil sensitivity distribution generating unit 42.

In the step S2, the RF coil sensitivity distribution generating unit 42 acquires the raw data provided through the sequence controller control unit 41 from the sequence controller 31 and arranges the acquired raw data in K-space (Fourier space), and also generates a RF coil sensitivity map of the RF coil 24 by performing known signal processing, for generating a RF coil sensitivity map, of the arranged raw data. For example, the RF coil sensitivity map can be generated by obtaining a signal intensity corresponding to each position on image data derived by image reconstruction processing of the raw data. Then, the RF coil sensitivity distribution generating unit 42 generates a RF coil sensitivity distribution indicating a change of signal intensity in an encode direction based on each signal intensity on the generated RF coil sensitivity map.

FIG. 9 is a diagram showing a RF coil sensitivity distribution generated by the RF coil sensitivity distribution generating unit 42 shown in FIG. 7.

As shown in FIG. 9 for example, a signal intensity corresponding to each acquisition position by the RF coil 24 is represented as a graph.

The RF coil sensitivity distribution generating unit 42 provides data including the generated RF coil sensitivity distribution to the storage unit 36.

In the step S3, the storage unit 36 acquires the data including the RF coil sensitivity distribution provided from the RF coil sensitivity distribution generating unit 42, and stores the acquired data including the RF coil sensitivity distribution. The data with regard to the RF coil sensitivity distribution includes not only data indicating a signal intensity corresponding to each acquisition position but also data indicating a voxel size used for acquiring the data for generating the RF coil sensitivity distribution and data indicating the number-of-times-of-integration of signals which are integrated for generating the RF coil sensitivity distribution, for example.

FIG. 10 is a flowchart explaining processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit 43 shown in FIG. 7.

The processing for calculating the number-of-times-of-integration by the magnetic resonance imaging apparatus 20 in FIG. 7 will be described with reference to the flowchart in FIG. 10. The processing for calculating the number-of-times-of-integration is started before performing a MRS scan (examination) actually through an operation of the input device 33 by an operator, for example when an instruction for starting a ¹H-MRS scan in a desired MRS target region is received by the sequence controller control unit 41.

In the step S11, the sequence controller control unit 41 determines whether an instruction for starting a ¹H-MRS scan in a desired MRS target region is received through an operation of the input device 33 by an operator, for example, and waits until it is determined that the instruction for starting a ¹H-MRS scan in the desired MRS target region (MRS acquisition region) is received.

In the step S11, when the sequence controller control unit 41 determined that an instruction for starting a ¹H-MRS scan in the desired MRS target region was received through an operation of the input device 33 by an operator, the sequence controller control unit 41 controls the sequence controller 31 before starting a ¹H-MRS scan in the desired MRS target region in the step S12 to acquire echo signals for generating image data used for a MRS plan and provides the acquired echo signals to the display data generating unit 44. The display data generating unit 44 acquires the echo signals, for a MRS plan image, provided from the sequence controller control unit 41 and displays a MRS plan image, generated by image reconstruction processing of the echo signals, on the display unit 34.

FIG. 11 is a diagram showing an example of displayed arbitrary image used for a plan on MRS.

The display unit 34 displays an arbitrary image used for a MRS plan as shown in FIG. 11. Then, an operator can set a voxel as a MRS target region by inputting information into the sequence controller control unit 41 through an operation of the input device 33.

After setting a MRS target region, the display data generating unit 44 displays the MRS target region as a single voxel superimposed on the plan image, Note that, in a case where multi voxels were set, local excitation regions are superimposed on the plan image.

In the step S13, the number-of-times-of-integration calculation unit 43 retrieves the data including the RF coil sensitivity distribution stored in the storage unit 36 before MRS imaging. The data including the RF coil sensitivity distribution includes the data indicating the signal intensity corresponding to each acquisition position, such as the signal intensity at the acquisition position at which the sensitivity is highest, and the data indicating the voxel size having been used in the data acquisition and the number-of-times-of-integration of the signals, like the voxel size N=8 (cc) and the number-of-times-of-integration (or the-number-of-times of the phase encodes) O=128.

In the step S14, the display data generating unit 44 retrieves the data including the RF coil sensitivity distribution stored in the storage unit 36, for calculation processing of the number-of-times-of-integration by the number-of-times-of-integration calculation unit 43, and displays the RF coil sensitivity distribution on the display unit 34 according to the retrieved data including the RF coil sensitivity distribution by controlling the display unit 34.

FIG. 12 is a diagram explaining a method for calculating the appropriate number of times of integrations corresponding to a size of a desired MRS target region.

The display unit 34 displays a RF coil sensitivity distribution as shown in FIG. 12, for example according to the control of the display data generating unit 44. In the RF coil sensitivity distribution in FIG. 12, the highest signal intensity in the entire arbitrary image for the MRS plan is regarded as M and the signal intensity at the MRS acquisition position is regarded as a.

In the step S15, the number-of-times-of-integration calculation unit 43 calculates the appropriate number-of-times of integrations, of echo signals for generating a spectrum, corresponding to the size of the desired MRS target region by a predetermined calculation method based on the retrieved data including the RF coil sensitivity distribution before MRS imaging.

Now, a method of calculating the appropriate number-of-times of integrations corresponding to the size of the desired MRS target region will be described with reference to FIG. 12. As shown in FIG. 12 for example, the highest signal intensity in the entire arbitrary image used for the MRS plan is regarded as M and the signal intensity at the MRS acquisition position is regarded as a. Then, the appropriate number-of-times of integrations (for multi voxels, a product of the number of the phase encodes and the number-of-times of integrations) X corresponding to the size of the desired MRS target region can be calculated by the expression (1) wherein the voxel size used for the MRS examination is q (cc) a reference voxel size corresponding to the position at which the sensitivity is highest is N (cc) and the reference number-of-times of integrations, of echo signals, corresponding to the position at which the sensitivity is highest is O.

X=(N/q)²×(M/a)² ×O  (1)

The number-of-times-of-integration calculation unit 43 provides the data including the calculated number-of-times of integrations to the sequence controller control unit 41.

Subsequently in the step S16, the sequence controller control unit 41 acquires the data including the number-of-times of integrations provided from the number-of-times-of-integration calculation unit 43, and makes the sequence controller 31 perform a MRS by providing a sequence of ¹H-MRS in the desired MRS target region (MRS acquisition region) based on the acquired data including the number-of-times of integrations to the sequence controller 31. That is, the sequence controller control unit 41 makes the sequence controller 31 apply radio frequency pulses and gradient magnetic field pulses to the object P in the static magnetic field and acquire magnetic resonance signals from a metabolite present in the object P.

Subsequently, the sequence controller control unit 41 provides the acquired magnetic resonance signals and the number of times of integrations to the display data generating unit 44. The display data generating unit 44 generates a frequency spectrum by integrating the magnetic resonance signals the number of times of integrations. Then, the generated frequency spectrum is displayed on the display unit 34. Thus, a spectrum having a narrow line width with a satisfactory S/N ratio can be acquired by the MRS examination.

By the magnetic resonance imaging apparatus 20 as described above, the appropriate number-of-times of integrations corresponding to a size of a desired MRS target region can be calculated so as to prevent an examination time from increasing unnecessarily for the reason that an actual examination results in failure or an examination time increases unnecessarily by a body motion even when a sensitivity of the RF coil 24 or a susceptibility of an object is not uniform. Therefore, a spectrum can be acquired in the minimum time and a waste of an examination time with MRS can be favorably eliminated.

Note that, in the embodiment of the present invention, the number-of-times of integrations used for acquiring magnetic resonance signals from a metabolite present in an object P is calculated. However, it is not limited to the above-described case. For example, the number of the phase encodes applied for acquiring data for generating a frequency spectrum may be calculated.

Further, the number-of-times-of integrations corresponding to a size of a MRS target region may be calculated based on a magnetic field uniformity distribution generated before MRS imaging as well as a RF coil sensitivity distribution generated in advance. The second embodiment of the present invention using this method will be described below.

2. SECOND EMBODIMENT

FIG. 13 is a functional block diagram of computer included in a magnetic resonance imaging apparatus according to a second embodiment of the present invention.

In FIG. 13, the same signs are attached with the respective elements, corresponding to those of the magnetic resonance imaging apparatus 20 shown in FIG. 7, as those shown in FIG. 7 and descriptions of them are omitted. The basic configurations of the magnetic resonance imaging apparatus is similar to those explained with referring to FIGS. 1 to 6 in the first embodiment of the present invention. Therefore, explanations of them are omitted.

The magnetic field uniformity distribution generating unit 45 acquires data for calculating a magnetic field uniformity provided through the sequence controller control unit 41 from the sequence controller 31, generates a magnetic field uniformity distribution by performing predetermined signal processing of the data for calculating a magnetic field uniformity, and provides data including the generated magnetic field uniformity distribution to the storage unit 36.

FIG. 14 is a flowchart explaining processing for generating a uniformity distribution of a magnetic field in the magnetic resonance imaging apparatus shown in FIG. 13.

The processing for generating a magnetic field uniformity distribution by the magnetic resonance imaging apparatus 20 in FIG. 13 will be described with reference to the flowchart in FIG. 14.

In the step S21, the sequence controller control unit 41 controls the sequence controller 31 to acquire echo data for calculating a magnetic field uniformity before MRS imaging. The sequence controller control unit 41 provides the acquired echo data for calculating a magnetic field uniformity to the magnetic field uniformity distribution generating unit 45.

In the step S22, the magnetic field uniformity distribution generating unit 45 acquires the echo data for calculating a magnetic field uniformity provided through the sequence controller control unit 41 from the sequence controller 31, calculates magnetic field uniformities in an entire image by performing known magnetic-field-uniformity-calculation-signal-processing of the echo data for calculating a magnetic field uniformity, and generates a magnetic field uniformity distribution.

For example, the magnetic field uniformity distribution can be calculated by measuring phase shifts of echo data or positional shifts of image data obtained from the echo data, due to magnetic field nonuniformity.

FIG. 15 is a diagram showing a magnetic field uniformity distribution generated by the magnetic field uniformity distribution generating unit 45 shown in FIG. 13.

As shown in FIG. 15, magnetic field uniformities corresponding to respective acquisition positions are displayed as a graph, for example.

The magnetic field uniformity distribution generating unit 45 provides the generated data including the magnetic field uniformity distribution to the storage unit 36.

In the step S23, the storage unit 36 acquires the data including the magnetic field uniformity distribution from the magnetic field uniformity distribution generating unit 45 and stores the acquired data including the magnetic field uniformity distribution. The data including the magnetic field uniformity distribution includes data indicating the magnetic field uniformities corresponding to the respective acquisition positions, for example.

FIG. 16 is a flowchart explaining processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit 43 shown in FIG. 13.

The processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit 43 shown in FIG. 13 will be described with referring to the flowchart of FIG. 16. Note that, the respective pieces of processing of the steps S31 to S35 of FIG. 16 are basically similar to those of the steps S11 to S15 of FIG. 10. Therefore, explanations of them are omitted. Note that, the first number-of-times-of-integration X corresponding to a desired size of a MRS target region is calculated by processing of the step S35.

In the step S36, the number-of-times-of-integration calculation unit 43 retrieves the data including the magnetic field uniformity distribution stored in the storage unit 36.

In the step S37, the display data generating unit 44 retrieves the data including the magnetic field uniformity distribution stored in the storage unit 36 for calculation processing of the number-of-times of integrations by the number-of-times-of-integration calculation unit 43, and controls the display unit 34 to display the magnetic field uniformity distribution on the display unit 34 based on the retrieved the data including the magnetic field uniformity distribution. That is, the display unit 34 displays the magnetic field uniformity distribution as shown in FIG. 12 according to the control of the display data generating unit 44, for example.

FIG. 17 is a diagram explaining a method for calculating the appropriate number of times of integrations corresponding to a size of a desired MRS target region.

In the magnetic field uniformity distribution in FIG. 17, the highest magnetic field uniformity in the entire arbitrary image used for a MRS plan is regarded as P (ppm) and the magnetic field uniformity at a MRS acquisition position is regarded as b (ppm). When the magnetic field uniformity is poor, a line width of a spectrum increases and a signal intensity decreases since the area is constant.

In the step S38, the number-of-times-of-integration calculation unit 43 calculates the second number-of-times of integrations corresponding to the size of the desired MRS target region by a predetermined calculation method based on the retrieved data including the magnetic field uniformity distribution before MRS imaging.

Now, a method of calculating the second number-of-times of integrations corresponding to the size of the desired MRS target region will be described with reference to FIG. 17. As shown in FIG. 17 for example, the highest magnetic field uniformity in the entire arbitrary image used for a MRS plan is regarded as P (ppm) and the magnetic field uniformity at the MRS acquisition position is regarded as b (ppm).

At this time, the second number-of-times of integrations (for multi voxels, a product of the number of the phase encodes and the number-of-times of integrations) Y corresponding to the size of the desired MRS target region can be calculated by the expression (2) using the number-of-times of integrations (the first number-of-times of integration) X calculated as described above.

Y=(P/b)² ×X  (2)

The number-of-times-of-integration calculation unit 43 provides the data including the calculated number-of-times of integrations to the sequence controller control unit 41.

Subsequently, in the step S39, the sequence controller control unit 41 acquires the data including the second number-of-times of integrations provided from the number-of-times-of-integration calculation unit 43, provides a sequence of ¹H-MRS, in the desired MRS target region (MRS acquisition region), based on the acquired data including the second number-of-times of integrations to the sequence controller 31 to perform MRS. That is, the sequence controller control unit 41 makes the sequence controller 31 apply radio frequency pulses and gradient magnetic field pulses to an object P in the static magnetic field and acquire magnetic resonance signals from a metabolite present in the object P.

Subsequently, the sequence controller control unit 41 provides the acquired magnetic resonance signals and the number-of-times of integrations to the display data generating unit 44. The display data generating unit 44 generates a frequency spectrum by integrating magnetic resonance signals the number-of-times of integrations. Thus, a spectrum having a narrow line width with a satisfactory S/N ratio can be acquired by a MRS examination.

Note that, there is a method for using a line width of a spectrum acquired without water suppression before ¹H-MRS imaging for acquiring signals from a single region, as a method for using a corrected magnetic field uniformity. In this case, the number-of-times of integrations (for multi voxels, the product of the number of the phase encodes and the number-of-times of integrations) Y′ can be calculated by the expression (3) wherein a half value width of a water spectrum corresponding to the highest signal intensity M in the entire arbitrary image used for a MRS plan is S (ppm) and a half value width of the water spectrum of in a desired MRS target region is t (ppm).

Y′=(S/t)² ×X  (3)

The number-of-times of integrations can be calculated using both a RF coil sensitivity distribution and a magnetic field uniformity distributions or using only a magnetic field uniformity distribution.

That is, the number of times of integrations or the number of times of phase encodes can be set according to a factor or factors each influencing a frequency spectrum, such as a RF coil sensitivity distribution and/or a magnetic field uniformity distribution. Note that, each order in the expressions (1) to (2) may be an arbitrary positive value other than two. Therefore, the number of times of integrations Z can be calculated by the generalized expression (4) or (5).

Z=a ₁(N/q)^(n1) ·a ₂(M/a)^(n2) ·a ₃(P/b)^(n3) ·O  (4)

Z=b ₁(N/q)^(m1) ·b ₂(M/a)^(m2) ·b ₃(S/t)^(m3) ·O  (5)

wherein

Z: the number-of-times-of-integration;

N: a reference voxel size;

q: a voxel size of a MRS target region;

M: the maximum signal intensity on a plan image;

a: a signal intensity on a position for MRS acquisition;

P: the maximum value of index representing magnetic field uniformity on the plan image;

b: an index representing magnetic field uniformity on the position for MRS acquisition;

S: a half-value width of a reference water spectrum;

t: a half-value width of a water spectrum on the position for MRS acquisition;

O: the reference number-of-times-of-integration;

a₁, a₂, a₃, b₁, b₂ and b₃ (>0) : coefficients; and

n1 n2, n3, m1, m2 and m3: positive values.

The reference voxel size N, the half-value width of a reference water spectrum S and the reference number-of-times-of-integration O can be set to values corresponding to the maximum sensitivity and the maximum magnetic field uniformity. The coefficients a₁, a₂, a₃, b₁, b₂ and b₃ and the positive values n1, n2, n3, m1, m2 and m3 can be set to appropriate values obtained experimentally or experientially. Each of the positive values n1, n2, n3, m1, m2 and m3 can be set to not only an integer such as 0, 1, 2 or 3 but also a value such as ½ or ⅓.

As shown in the expressions (4) and (5), the number of times of integrations Z becomes larger when q, a, b and/or t are relatively smaller to N, M, P and/or S respectively.

Alternatively, by referring to a table derived by previously relating the appropriate numbers of times of integrations with respective values of each parameter such as a voxel size which influences a frequency spectrum, instead of using a expression like the expression (4) or (5), the number of times of integrations corresponding to values of the respective parameters may be set as one for MRS. In this case, the table can be stored in the storage unit 36.

Note that, the number of times of phase encodes can be determined by a similarly method.

By the way, while the sequence controller control unit 41 performs a MRS examination, the display unit 34 displays a spectrum derived by the MRS examination according to the control of the display data generating unit 44. Conventionally, processing for displaying a spectrum is performed after MRS acquisition. For this reason, a SNR might be insufficient although the MRS examination was performed. In such a case, to improve the SNR later takes an extra time. For that reason, the display data generating unit 44 performs processing for generating and displaying a MRS spectrum to display the MRS spectrum on the display unit 34 during a set MRS observation time according to the control of the sequence controller control unit 41.

FIG. 18 shows an example of configuration of a touch panel displayed for acquisition by MRS.

FIG. 18 (A) shows a spectrum, which is being acquired, of a single voxel after a lapse of 1 minute, and FIG. 18 (B) shows a spectrum, which is being acquired, of the single voxel after a lapse of 4 minutes.

Of course, processing for displaying a spectrum may be performed per single integration in MRS. In a case of ¹H-MRS (proton spectroscopy), processing for displaying a spectrum may be performed per multiple-of-eight times of integrations when the spectrum without water suppression is acquired with eight integrations for example.

As shown in (A) and (B) of FIG. 18, a touch panel 51 as input means Carl be displayed simultaneously when a MRS spectrum is displayed on the display unit 34. As shown in (A) and (B) of FIG. 18, for example, the touch panel 51 includes a Save&Exit button 51-1 having the function to quit an imaging on the way and save (store) a spectrum in case where a SNR is sufficient, an Abort button 51-2 having the function to quit an imaging on the way in case where a desired spectrum can not be acquired and a Change button 51-3 having the function to change the number-of-times of integrations on the way in case where the set number-of-times of integrations seems to be insufficient. Therefore, conditions for acquiring a frequency spectrum can be changed on acquisition of the frequency spectrum by operating the touch panel 51.

Accordingly, for example, when a SNR of a spectrum is sufficient during execution of a MRS with the calculated number-of-times of integrations, the MRS imaging can be aborted on the way and data can be saved (stored) in the storage unit 36 with an operation of the Save&Exit button 51-1 by an operator. On the contrary, when a desired spectrum does not seem to be acquired during acquisition, the imaging that does not acquire a desired spectrum can be quitted with an operation of the Abort button 51-2 by an operator.

Alternatively, for example, in case where the set number-of-times of integrations seems to be insufficient during execution of a MRS with the calculated number-of-tines of integrations, the number-of-times of integrations can be changed on acquisition of a spectrum with an operation of the Change button 51-3 by an operator. Of course, this change function can be performed after completion of the MRS imaging. Specifically, after completion of the MRS imaging with the number-of-times of integrations (e.g., 128 times) calculated and set according to the flowchart in FIG. 10 or FIG. 16, the number-of-times of integrations can be changed to 192 times so that 64 times data acquisitions are performed additionally, for example. In this case, pieces of data corresponding to 192 integrations are acquired to be processed.

Note that, dedicated input buttons can be provided as a part of the input device 33 in place of the touch panel.

The third embodiment of the present invention using this method will be described below.

By the way, it is possible to determine a body motion of an object P per preset number-of-times of integrations based on phase shifts of echo signals derived by acquiring a spectrum of water according to the gradient echo method or the like and also alert an operator that at least one of the phase shifts of the echo signals exceeds a constant amount and excess of the phase shift continues not less than a constant. period of time in such a case.

3. THIRD EMBODIMENT

FIG. 19 is a functional block diagram of computer included in a magnetic resonance imaging apparatus according to a third embodiment of the present invention.

In FIG. 19, the same signs are attached with the respective elements, corresponding to those of the magnetic resonance imaging apparatus 20 shown in FIG. 7, as those shown in FIG. 7 and descriptions of them are omitted. The basic configurations of the magnetic resonance imaging apparatus is similar to those explained with referring to FIGS. 1 to 6 in the first embodiment of the present invention. Therefore, explanations of them are omitted.

The sequence controller control unit 41 make the sequence controller 31 acquire NMR signals for MRS and correction signals for correcting a spectrum per the preset number-of-times of integrations from a region including at least a MRS target region by the gradient echo.

The correction signal analysis unit 52 acquires the correction signals provided through the sequence controller control unit 41 from the sequence controller 31 per the preset number-of-times of integrations, and also analyzes the acquired correction signals by performing predetermined signal processing of the correction signals. Then, a body motion of an object P can be detected by determining whether each phase shift of the correction signals is not less than a constant amount. When the correction signal analysis unit 52 determines that a phase shift of at least one correction signal is not less than the constant amount as a result of analysis of the correction signals, the correction signal analysis unit 52 recognizes a body motion of the object P and generates a detection signal. The generated detection signal is supplied to the sequence controller control unit 41 and the display data generating unit 44.

FIG. 20 is a flowchart explaining processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit 43 shown in FIG. 19.

The processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit 43 shown in FIG. 19 will be described with referring to the flowchart of FIG. 20. Note that, the respective pieces of processing of the steps S51 to S55 of FIG. 20 are basically similar to those of the steps S11 to S15 of FIG. 10. Therefore, explanations or them are omitted.

In the step S56, the sequence controller control unit 41 acquires data including the number-of-times of integrations provided from the number-of-times-of-integration calculation unit 43, and provides a ¹H-MRS sequence for a desired MRS target region (MRS acquisition region) based on the acquired data including the number-of-times of integrations to the sequence controller 31 so that MRS starts.

In the step S57, the sequence controller control unit 41 make the sequence controller 31 acquire the correction signals for a MRS spectrum from a predetermined region for correction signal acquisition including at least a MRS target region as shown in FIG. 21 per the preset number-of-times of integrations.

FIG. 21 is a diagram showing a specified region, which includes a MRS target region, for acquiring correction signals.

Note that, in the case of FIG. 21, a cross-section for acquiring data is an axial cross section, However, the cross-section for acquiring data Nay be a sagittal section or a coronal section.

In the step S58, the correction signal analysis unit 52 acquires the correction signals provided through the sequence controller control unit 41 from the sequence controller 31 per the preset number-of-times of integrations, and also determines whether a phase shift of at least one correction signal is not less than a constant amount by performing predetermined signal processing of the correction signals for analysis.

FIG. 22 is a diagram showing a phase shift of correction signal.

Each of (A) and (B) in FIG. 22 shows phase shifts of the correction signals. As shown in (A) and (B) of FIG. 22, when an initial phase is a and an acceptable range of a phase shift is φ (20° for example), a body motion of an object P occurs at the t-th integration (t-th encode for multi voxels) and a phase deviates to e beyond the acceptable range. Therefore, it is determined that a phase shift of a correction signal is not less than a constant amount in both (A) and (B) of FIG. 22.

In the step S58, when the correction signal analysis unit 52 determines that a phase shift of a correction signal is not less than the constant amount, the correction signal analysis unit 52 detects a body motion of an object P and generates a detection signal according to the body motion of the object P in the step 359.

That is, in the case of (A) in FIG. 22, the phase deviated to e beyond the acceptable range once and subsequently returned to the former phase because the body motion of the object P is instantaneous. For that reason, the correction signal analysis unit 52 generates a detection signal indicating that the data corresponding to the part having moved is to be excluded from processing with continuing the MRS acquisition for the single voxel so that data corresponding to a part having moved should be excluded from processing with continuing MRS acquisition for a single voxel. The generated detection signal is provided to the sequence controller control unit 41. Note that, in the case of MRS for multi voxels, the correction signal analysis unit 52 generates a detection signal indicating that encode data during a body motion of the object P should be reacquired. Then, the generated detection signal is provided to the sequence controller control unit 41.

On the other hands, in the case of (B) in FIG. 22, a body motion of the object P is not instantaneous, and therefore, the phase does not return to the former phase after the phase deviated to e beyond the acceptable range once. Accordingly in the case of (B) in FIG. 22, the body motion of the object P is too large to disregard influence on the MRS examination. For that reason, the correction signal analysis unit 52 generates a detection signal for displaying a message that a body motion of the object P was detected on the display unit 34 and provides the generated detection signal to the display data generating unit 44 so that the message that the body motion of the object P was detected is displayed on the display unit 34.

On the other hands, when the correction signal analysis unit 52 determines that each of the phase shifts of the correction signals is less than the constant amount in the step S58, the processing of the step S59 is skipped and the correction signal analysis unit 52 does not generate any detection signal.

In the step S60, the sequence Controller control unit 41 provides a ¹H-MRS sequence for a desired MRS target region (MRS acquisition region) based on the acquired data including the number-of-times of integrations to the sequence controller 31 so that the sequence controller 31 performs a MRS. That is, radio frequency pulses and gradient magnetic field pulses are applied to an object P in a static magnetic field to acquire magnetic resonance signals from a metabolite present in the object P.

Then, in the case of (A) in FIG. 22, the phase returns to the former phase after the phase deviated to e beyond the acceptable range once because the body motion of the object P was instantaneous. For that reason, the sequence controller control unit 41 excludes data during the body motion from processing with continuing MRS acquisition for a single voxel based on the detection signal provided from the correction signal analysis unit 52. Accordingly, not only a spectrum having narrow line widths can be acquired with a satisfactory S/N ratio by a MRS examination, but also an influence of a body motion of an object P on the MRS examination can be excluded even if the body motion of the object P occurred.

On the other hands, in the case of (B) in FIG. 22, a body motion of the object P was not instantaneous, and therefore, the phase does not return to the former phase after the phase deviated to e beyond the acceptable range. Consequently, the body motion of the object P is too large to disregard an influence on the MRS examination. For that reason, the display data generating unit 44 controls the display unit 34 so as to display a message indicating that a body motion of the object P was detected on the display unit 34 according to the detection signal provided from the correction signal analysis unit 52. For example, a message such as “a body motion of the object P occurred” is displayed on the display unit 34. This allows an operator to notice that a body motion of the object P occurred during the MRS examination. Then, the operator can quit the MRS examination afterward through an operation of the input device 33. Note that, an operator can be informed of a message by voice or with light emitting elements.

In the step S61, the sequence controller control unit 41 determines whether MRS was performed up to the calculated number-of-times of integrations. When the sequence controller control unit 41 determines that MRS was performed up to the calculated number-of-times of integrations in the step S61, the processing proceeds to the step S62. The sequence controller control unit 41 quits the MRS execution in the step S62.

On the other hands, in the step S61, when the sequence controller control unit 41 determines that MRS has not been performed up to the calculated number-of-times of integrations yet, the sequence controller control unit 41 increments the number-of-times of integration by 1. Subsequently, the processing returns to the step S57, the processing on and after the step S57 is performed repeatedly. This allows the MRS to be performed up to the calculated number-of-times of integrations to acquire data.

The third embodiment of the present invention can not only calculate the appropriate number-of-times of integrations corresponding to a size of a desired MRS target region, but also, prevent an examination time from increasing unnecessarily for the reason that an actual examination results in failure by a body motion or an examination time increases unnecessarily even when a sensitivity of a RF coil 24 or a susceptibility of an object is not uniform. In addition, even if a body motion of an object P occurs during a MRS examination, data during the body motion can be excluded from processing and an operator can be informed of a message that the body motion of the object P was detected. Therefore, the waste of the examination time with MRS can be favorably eliminated.

Note that, amplitudes (signal intensities) of correction signals can be used instead of phases of correction signals. Alternatively, both amplitudes and phases of correction signals can be used. In the flowchart in the FIG. 20, a body motion of an object P is determined per the preset number-of-times of integrations based on phase shifts of echo signals after acquiring a spectrum of water with a method such as the gradient echo method. However, not only this case, but a body motion of an object P can be detected per several integrations (per several encodes for multi voxels), for example.

FIG. 23 is a diagram showing a shift in center frequency of correction signal with time.

As shown in FIG. 23, when an initial center frequency is f and an acceptable range of the center frequency is C (0.1 ppm, for example), the center frequency deviates from the acceptable range due to a change in temperature of a gradient magnetic field system and the like at the t-th integration (in the case of multi voxels, t-th encode).

FIG. 24 is a flowchart explaining another processing for calculating the number of times of integrations by the number-of-times-of-integration calculating unit 43 shown in FIG. 19.

As shown in the flowchart in FIG. 24, the correction signal analysis unit 52 determines whether the center frequency exceeds the acceptable range by at least a predetermined amount in the step S80. When the correction signal analysis unit 52 determines that the center frequency exceeds the acceptable range by at least the predetermined amount in the step S80, the sequence controller control unit 41 performs MRS with shifting the center frequency f to f+C and in the step S81. In the case of FIG. 23, for example, the center frequencies for MRS acquisition are shifted to f+C on and after (t+1)-th integration. Accordingly, a MRS examination can be favorably performed even when a gradient magnetic field changes with time.

Note that, processing in the steps S71 to S79 and the steps S82 to S84 in FIG. 24 are basically similar to processing in the steps S51 to S62 in FIG. 20. Therefore, a detailed explanation Is omitted.

A series of processing described in each embodiment of the present invention can be performed by software or hardware.

In each embodiment of the present invention, an example of processing in which the steps in each flowchart are performed in time series according to the described order is shown. However, the steps may not be processed in time series. That is, the respective steps may be performed in parallel or individually. 

1. A magnetic resonance imaging apparatus comprising: a spectrum acquisition unit configured to acquire a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and a determining unit configured to determine one of the number of times of integrations and the number of times of phase encodes of magnetic resonance signals for obtaining the frequency spectrum depending on a factor influencing the frequency spectrum.
 2. A magnetic resonance imaging apparatus comprising: a spectrum acquisition unit configured to acquire a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and an acquisition condition changing unit configured to change an acquisition condition of the frequency spectrum during acquiring the frequency spectrum.
 3. A magnetic resonance imaging apparatus of claim 1, wherein said determining unit is configured to determine the one depending on a sensitivity distribution of a radio frequency coil for receiving the magnetic resonance signals for obtaining the frequency spectrum.
 4. A magnetic resonance imaging apparatus of claim 3, further comprising: a sensitivity distribution acquisition unit configured to acquire the sensitivity distribution; and a display unit configured to display the sensitivity distribution.
 5. A magnetic resonance imaging apparatus of claim 1, wherein said determining unit is configured to determine the one depending on a magnetic field uniformity distribution.
 6. A magnetic resonance imaging apparatus of claim 5, further comprising: a magnetic field uniformity distribution acquisition unit configured to acquire the magnetic field uniformity distribution; and a display unit configured to display the magnetic field uniformity distribution.
 7. A magnetic resonance imaging apparatus of claim 1, wherein said determining unit is configured to determine the one depending on a size of the target region.
 8. A magnetic resonance imaging apparatus of claim 1, wherein said determining unit is configured to determine the one depending on a line width of a previously acquired frequency spectrum.
 9. A magnetic resonance imaging apparatus of claim 1, further comprising: an acquisition condition changing unit configured to change an acquisition condition of the frequency spectrum during acquiring the frequency spectrum.
 10. A magnetic resonance imaging apparatus of claim 2, wherein said acquisition condition changing unit includes a display part configured to display a frequency spectrum on acquisition.
 11. A magnetic resonance imaging apparatus of claim 2, wherein said acquisition condition changing unit includes an input part for changing one of the number of times of integrations and the number of times of phase encodes of magnetic resonance signals for obtaining the frequency spectrum.
 12. A magnetic resonance imaging apparatus of claim 2, wherein said acquisition condition changing unit includes an input part for aborting acquisition of the frequency spectrum.
 13. A magnetic resonance imaging apparatus of claim 2, wherein said acquisition condition changing unit includes: a storage part configured to save a frequency spectrum on acquisition; and an input part for aborting acquisition of the frequency spectrum.
 14. A magnetic resonance imaging apparatus of claim 1, further comprising: a correction signal acquisition unit configured to acquire correction signals from a region including at least the target region, wherein said spectrum acquisition unit is configured to generate the frequency spectrum with excluding a magnetic resonance signal acquired during a body movement by the object, the magnetic resonance signal acquired during the body movement being determined based on at least one of phase variations and amplitude variations of the correction signals.
 15. A magnetic resonance imaging apparatus of claim 1, further comprising: a correction signal acquisition unit configured to acquire correction signals from a region including at least the target region; and a warn unit configured to warn detection information of a body movement by the object in case where the body movement is detected based on at least one of phase variations and amplitude variations of the correction signals.
 16. A magnetic resonance imaging apparatus of claim 15, further comprising: an input unit for inputting information instructing whether acquisition of the frequency spectrum is to be aborted or to be continued in case where the detection information is warned by said warn unit.
 17. A magnetic resonance imaging apparatus of claim 1, further comprising: a correction signal acquisition unit configured to acquire correction signals from a region including at least the target region, wherein said spectrum acquisition unit is configured to shift at least one of center frequencies of the magnetic resonance signals from the metabolic product according to shift amounts of center frequencies of the correction signals in case where at least one of the shift amounts is not less than a predetermined amount.
 18. A magnetic resonance imaging method comprising: acquiring a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and determining one of the numbers of integrations and phase encodes of magnetic resonance signals for obtaining the frequency spectrum depending on a factor influencing the frequency spectrum.
 19. A magnetic resonance imaging method comprising: acquiring a frequency spectrum of magnetic resonance signals from a metabolic product in a target region in an object by applying radio frequency pulses and gradient magnetic field pulses to the object in a static magnetic field; and changing an acquisition condition of the frequency spectrum during acquiring the frequency spectrum. 